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2. Contributors

Author

Adams, Paul C., primary, Albrecht, Helmut, additional, Bajaj, Jasmohan, additional, Baik, Soon Koo, additional, Beuers, Ulrich, additional, Biggins, Scott W., additional, Bismuth, Henri, additional, Boberg, Kirsten Muri, additional, Bonkovsky, Herbert L., additional, Bosch, Jaime, additional, Boyer, Thomas D., additional, Brunt, Elizabeth M., additional, Caselitz, Martin, additional, Caselmann, Wolfgang H., additional, Cave, Matt, additional, Chan, Henry Lik-Yuen, additional, Chang, Kyong-Mi, additional, Ciancio, Alessia, additional, Colombo, Massimo, additional, Conjeevaram, Hari S., additional, Cox, Diane W., additional, Day, Chris P., additional, Doctor, R. Brian, additional, Oude Elferink, Ronald P.J., additional, Elisofon, Scott A., additional, El-Serag, Hashem B., additional, Esmat, Gamal, additional, Everson, Gregory T., additional, Falkner, Keith Cameron, additional, Fallon, Michael B., additional, Feng, Sandy, additional, Fischer, Hans-Peter, additional, Fortune, Brett E., additional, Friedman, Scott L., additional, García-Pagán, J.C., additional, Garcia-Tsao, Guadalupe, additional, Ghishan, Fayez K., additional, Gores, Gregory J., additional, Gruessner, Rainer W., additional, Gupta, Sanjeev, additional, Hammoud, Ghassan M., additional, Heathcote, E.J., additional, Helmke, Steve M., additional, Hirschfield, G.M., additional, Hunt, Douglas, additional, Iavarone, Massimo, additional, Ibdah, Jamal A., additional, Imbert-Bismut, Françoise, additional, Jansen, Peter L.M., additional, Johnson, Benjamin F., additional, F. Jonas, Maureen M., additional, Jones, Dean P., additional, Kamath, Patrick S., additional, Karlsen, Tom H., additional, Kelly, Deirdre, additional, Kettelle, J., additional, Khan, Khalid M., additional, Knolle, Percy, additional, Kramer, David J., additional, Kumar, Manoj, additional, Kumar, Navaneeth C., additional, Lai, Jennifer C., additional, Lapointe, Réal, additional, Lazaridis, Konstantinos N., additional, Lechel, André, additional, Lee, Samuel S., additional, Lencioni, Riccardo, additional, Levy, Cynthia, additional, Lindor, Keith D., additional, Locarnini, Stephen, additional, Lok, Anna S.F., additional, Malhi, Harmeet, additional, Manns, Michael P., additional, Marrero, Jorge A., additional, McClain, Craig, additional, McCuskey, Robert, additional, McGovern, Barbara H., additional, McHutchison, John G., additional, Moradpour, Darius, additional, Navarro, Victor J., additional, Neuberger, James, additional, Nevah R., Moises I., additional, Nevzorova, Yulia A., additional, Patton, Heather M., additional, Penin, François, additional, Perlmutter, David, additional, Plessier, Aurélie, additional, Poynard, Thierry, additional, Puri, Puneet, additional, Rice, Charles, additional, Rizzetto, Mario, additional, Roberts, Eve A., additional, Rockey, Don C., additional, Roy-Chowdhury, Jayanta, additional, Roy-Chowdhury, Namita, additional, Rudolph, K. Lenhard, additional, Russo, Mark W., additional, Saab, Sammy, additional, Sanyal, Arun J., additional, Sarin, S.K., additional, Schrumpf, Erik, additional, Seeff, Leonard B., additional, Seijo, S., additional, Shah, Vijay H., additional, Shedlofsky, Steven I., additional, Shouval, Daniel, additional, Sirlin, Claude B., additional, Smith, Maxwell L., additional, Smorodinsky, Emmanuil, additional, Spengler, Ulrich, additional, Sterling, Richard K., additional, Stewart, Stephen F., additional, Strader, Doris B., additional, Strassburg, Christian P., additional, Stravitz, R. Todd, additional, Sud, Priti, additional, Sulkowski, Mark S., additional, Talwalkar, Jayant A., additional, Terrault, Norah A., additional, Tillmann, Hans L., additional, Trautwein, Christian, additional, Vagefi, Parsia A., additional, Valla, Dominique, additional, Wagner, Siegfried, additional, Warner, Nadia, additional, Wong, Vincent Wai-Sun, additional, and Zayed, Naglaa, additional

Published
2012
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4. Value of liver biopsy in the diagnosis of drug-induced liver injury.

Author

Ahmad J, Barnhart HX, Bonacini M, Ghabril M, Hayashi PH, Odin JA, Rockey DC, Rossi S, Serrano J, Tillmann HL, and Kleiner DE

Subjects
Biopsy, Humans, Risk Factors, Chemical and Drug Induced Liver Injury diagnosis, Chemical and Drug Induced Liver Injury etiology, Dyphylline
Abstract

Background & Aims: The utility of liver biopsy in diagnosing or staging idiosyncratic drug-induced liver injury (DILI) is unclear. The aim of this study was to determine whether liver histology impacted causality assessment in suspected DILI using a novel simulation model., Methods: Fifty patients enrolled in the DILI Network (DILIN) who had liver biopsies performed within 60 days of DILI onset were randomly selected. All had standard DILIN consensus causality scoring using a 5-point scale (1=definite, 2=highly likely, 3=probable, 4=possible, 5=unlikely) based on 6-month post-injury data. Three experienced hepatologists independently performed a causality assessment using redacted case records, with the biopsy and selected post-biopsy laboratory data removed. The 3 hepatologists also reviewed the liver histology with a hepatopathologist and then repeated causality assessment for each case., Results: Of the 50 cases, there were 42 high causality DILI cases (1, 2 or 3) and 8 low causality cases (4 and 5). The hepatologists judged that liver biopsy was indicated in 62% of patients; after histology review, biopsy was judged to have been helpful in 70% of patients. Histology review changed the causality score in 68% of patients, with an increase in DILI likelihood in 48% and a decrease in 20%. Biopsy results changed diagnostic certainty from less certain (3 or 4) to highly certain (1, 2 or 5) in 38% of patients., Conclusions: Liver histologic findings may help clarify the diagnosis of DILI. Histology appears to be particularly helpful in cholestatic or equivocal cases of DILI (possible or probable), shifting assessment toward a greater or lower certainty of a DILI diagnosis., Lay Summary: The utility of liver biopsy in diagnosing or staging idiosyncratic drug-induced liver injury (DILI) is unclear. Herein, we show that, in patients with suspected DILI, a liver biopsy can help physicians diagnose DILI or other causes of liver injury with more certainty., Competing Interests: Conflict of interest JA, HXB, MG, PHH, JAO, DR, SR, JS, DEK: No conflict of interest to disclose. MB: Speaker: Abbvie, Gilead, Intercept. Research support: Viking, Intercept, Boehringer-Ingelheim, Assembly Biosciences, Allergan, Genfit. HLT: Spouse is an Abbvie employee and holds stocks in Abbott, Abbvie, Gilead and HLT consulted for Trevena Inc. and Novo Nordisk. Please refer to the accompanying ICMJE disclosure forms for further details., (Copyright © 2022. Published by Elsevier B.V.)

Published
2022
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5. "On demand" sedation for colonoscopy with or without auricular acupuncture is non-inferior and may improve quality metrics compared to "upfront" sedation.

Author

Beacham MC, McMillen WP, Kirkman SS, Maxey DK, Freedman M, and Tillmann HL

Subjects
Conscious Sedation, Humans, Patient Preference, Quality Improvement, Retrospective Studies, Acupuncture Therapy, Colonoscopy methods, Pain Management methods
Abstract

Competing Interests: Declaration of Competing Interest No conflict of interest with this work. The views expressed in this article are those of the authors and do not necessarily reflect the position or policy of the Department of Veterans Affairs or the United States government.

Published
2021
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8. Genome-wide association study of interferon-related cytopenia in chronic hepatitis C patients.

Author

Thompson AJ, Clark PJ, Singh A, Ge D, Fellay J, Zhu M, Zhu Q, Urban TJ, Patel K, Tillmann HL, Naggie S, Afdhal NH, Jacobson IM, Esteban R, Poordad F, Lawitz EJ, McCone J, Shiffman ML, Galler GW, King JW, Kwo PY, Shianna KV, Noviello S, Pedicone LD, Brass CA, Albrecht JK, Sulkowski MS, Goldstein DB, McHutchison JG, and Muir AJ

Subjects
Adult, Antiviral Agents adverse effects, Female, Genome-Wide Association Study, Humans, Interferon alpha-2, Linkage Disequilibrium, Male, Middle Aged, Polymorphism, Single Nucleotide, Pyrophosphatases genetics, Recombinant Proteins adverse effects, Ribavirin adverse effects, Thrombocytopenia chemically induced, Thrombocytopenia genetics, Hepatitis C, Chronic drug therapy, Hepatitis C, Chronic genetics, Interferon-alpha adverse effects, Leukopenia chemically induced, Leukopenia genetics, Neutropenia chemically induced, Neutropenia genetics, Polyethylene Glycols adverse effects
Abstract

Background & Aims: Interferon-alfa (IFN)-related cytopenias are common and may be dose-limiting. We performed a genome wide association study on a well-characterized genotype 1 HCV cohort to identify genetic determinants of peginterferon-α (pegIFN)-related thrombocytopenia, neutropenia, and leukopenia., Methods: 1604/3070 patients in the IDEAL study consented to genetic testing. Trial inclusion criteria included a platelet (Pl) count ≥80×10(9)/L and an absolute neutrophil count (ANC) ≥1500/mm(3). Samples were genotyped using the Illumina Human610-quad BeadChip. The primary analyses focused on the genetic determinants of quantitative change in cell counts (Pl, ANC, lymphocytes, monocytes, eosinophils, and basophils) at week 4 in patients >80% adherent to therapy (n=1294)., Results: 6 SNPs on chromosome 20 were positively associated with Pl reduction (top SNP rs965469, p=10(-10)). These tag SNPs are in high linkage disequilibrium with 2 functional variants in the ITPA gene, rs1127354 and rs7270101, that cause ITPase deficiency and protect against ribavirin (RBV)-induced hemolytic anemia (HA). rs1127354 and rs7270101 showed strong independent associations with Pl reduction (p=10(-12), p=10(-7)) and entirely explained the genome-wide significant associations. We believe this is an example of an indirect genetic association due to a reactive thrombocytosis to RBV-induced anemia: Hb decline was inversely correlated with Pl reduction (r=-0.28, p=10(-17)) and Hb change largely attenuated the association between the ITPA variants and Pl reduction in regression models. No common genetic variants were associated with pegIFN-induced neutropenia or leucopenia., Conclusions: Two ITPA variants were associated with thrombocytopenia; this was largely explained by a thrombocytotic response to RBV-induced HA attenuating IFN-related thrombocytopenia. No genetic determinants of pegIFN-induced neutropenia were identified., (Copyright © 2011 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published
2012
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9. The predictive value of IL28B gene polymorphism for spontaneous clearance in a single source outbreak cohort is limited in patients carrying the CCR5Δ32 mutation.

Author

Nattermann J, Timm J, Nischalke HD, Olbrich A, Michalk M, Tillmann HL, Berg T, Wedemeyer H, Tenckhoff H, Wiese M, Kullig U, Göbel U, Capka E, Schiefke I, Güthof W, Grüngreiff K, König I, Roggendorf M, Sauerbruch T, and Spengler U

Subjects
Alleles, Case-Control Studies, Cohort Studies, Disease Outbreaks, Drug Contamination, Female, Gene Frequency, Genotype, Germany epidemiology, Hepatitis C epidemiology, Hepatitis C immunology, Hepatitis C transmission, Hepatitis C virology, Humans, Interferons, Polymorphism, Single Nucleotide, Sequence Deletion, Hepatitis C genetics, Interleukins genetics, Receptors, CCR5 genetics
Abstract

Background & Aims: The CCR5Δ32 mutation has been suspected to adversely affect outcomes of HCV infection, although reports have remained controversial. Here, we investigated the relative genetic contributions of the CCR5Δ32 deletion and the IL28B rs12979860 polymorphisms to spontaneous clearance of hepatitis C in a single-source outbreak., Methods: We retrieved 396 Caucasian women (119 women with spontaneous HCV clearance) who had been infected with HCV genotype 1-contaminated anti-D immunoglobulin in 1978, and determined their IL28B and CCR5 alleles., Results: IL28B CC, CT, and TT genotypes were found in 35.4%, 50%, and 14.6% of patients and corresponded to spontaneous clearance rates of 50%, 21.2%, and 12.1% (Chi(2)=38.7, p=5.0×10(-10)), respectively. CCR5 WT/WT, WT/Δ32, and Δ32/Δ32 genotypes were observed in 76%, 22.7%, and 1.3% of patients and corresponded to clearance rates of 33.2%, 21.2%, and 0% (Chi(2)=6.9, p=0.009), respectively. In a stepwise forward-conditional multivariate regression model both CCR5 (OR 2.1, p=0.01 for WT/WT) and IL28B genetic variants (OR 4.3, p=4.6×10(-10) for the C/C genotype) were identified as independent predictors of spontaneous HCV clearance. Importantly, favorable response rates were associated with the IL28B CC genotype only in CCR5 wild-type homozygous women, while HCV clearance in CCR5Δ32 carriers remained poor even in patients with the rs12979860 CC genotype., Conclusions: Both IL28B rs1297860 and CCR5Δ32 allelic variants are independent genetic determinants of spontaneous HCV clearance. The variable relative distribution between IL28B rs1297860 and CCR5Δ32 allelic variants in different populations may have masked the role of the CCR5Δ32 mutation in some studies., (Copyright © 2011 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published
2011
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10. Beneficial IL28B genotype associated with lower frequency of hepatic steatosis in patients with chronic hepatitis C.

Author

Tillmann HL, Patel K, Muir AJ, Guy CD, Li JH, Lao XQ, Thompson A, Clark PJ, Gardner SD, McHutchison JG, and McCarthy JJ

Subjects
Adult, Antiviral Agents administration & dosage, Cohort Studies, Fatty Liver metabolism, Female, Genetic Predisposition to Disease, Genotype, Hepatitis C, Chronic drug therapy, Hepatitis C, Chronic metabolism, Humans, Interferons, Lipid Metabolism genetics, Lipoproteins blood, Male, Middle Aged, Treatment Outcome, Fatty Liver etiology, Fatty Liver genetics, Hepatitis C, Chronic complications, Hepatitis C, Chronic genetics, Interleukins genetics, Polymorphism, Single Nucleotide
Abstract

Background & Aims: IL28B polymorphisms have been associated with both treatment induced and spontaneous clearance of hepatitis C virus (HCV). We previously found that LDL cholesterol levels were higher in chronic hepatitis C (CHC) patients with the CC genotype at the rs12979860 polymorphism, located proximal to the IL28 gene. Here we analyzed the association of steatosis with IL28B genotype in treatment naïve patients with CHC., Methods: Two independent cohorts of 145 genotype 1 infected patients from an antifibrotic study and 180 genotype 1 patients from Duke were analyzed for the presence and severity of steatosis in relation to the rs12979860 polymorphism at the IL28B locus. TaqMan assay based genotyping classified three groups CC, CT, and TT., Results: CC genotype was associated with a lower prevalence of steatosis. In the antifibrotic study, steatosis was found in 47.6% (50/105) of IL28B non-CC vs. 22.5% (9/40; p=0.008) in CC patients. Similarly, steatosis was found in 67.4% (89/132) of non-CC patients compared to only 39.6% (19/48; p=0.001) of CC patients in the Duke cohort., Conclusions: IL28B CC genotype is associated with less pronounced disturbances of lipid metabolism, as reflected both in serum lipoprotein levels and hepatic steatosis, in HCV infection., (Copyright © 2011 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published
2011
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11. Hepatitis B surface antigen quantification: why and how to use it in 2011 - a core group report.

Author

Chan HL, Thompson A, Martinot-Peignoux M, Piratvisuth T, Cornberg M, Brunetto MR, Tillmann HL, Kao JH, Jia JD, Wedemeyer H, Locarnini S, Janssen HL, and Marcellin P

Subjects
Antiviral Agents therapeutic use, Biomarkers blood, Hepatitis B virus physiology, Hepatitis B, Chronic virology, Humans, Interferon-alpha therapeutic use, Polyethylene Glycols therapeutic use, Prognosis, Recombinant Proteins therapeutic use, Reverse Transcriptase Inhibitors therapeutic use, Hepatitis B Surface Antigens blood, Hepatitis B e Antigens blood, Hepatitis B virus immunology, Hepatitis B, Chronic diagnosis, Hepatitis B, Chronic drug therapy
Abstract

Quantitative HBsAg had been suggested to be helpful in management of HBV, but assays were cumbersome. The recent availability of commercial quantitative assays has restarted the interest in quantitative serum hepatitis B surface antigen (HBsAg) as a biomarker for prognosis and treatment response in chronic hepatitis B. HBsAg level reflects the transcriptional activity of cccDNA rather than the absolute amount of cccDNA copies. Serum HBsAg level tends to be higher in hepatitis B e antigen (HBeAg)-positive than HBeAg-negative patients. Among patients with a low HBV DNA (<2000IU/ml), HBsAg <1000IU/ml in genotype D HBV infection and HBsAg <100IU/ml in genotype B/C HBV infection is associated with inactive carrier state in HBeAg-negative patients. The HBsAg reduction by nucleos(t)ide analogues (NA) is not as pronounced as by interferon treatment. On peginterferon treatment, sustained responders tend to show greater HBsAg decline than the non-responders. The optimal on-treatment HBsAg cutoff to predict response needs further evaluation in HBeAg-positive patients, but an absence of HBsAg decline together with a <2 log reduction in HBV DNA at week 12 can serve as stopping rule in HBeAg-negative patients with genotype D HBV infection. A rapid serum HBsAg decline during NA therapy may identify patients who will clear HBsAg in the long-term. There are early reports among Asian patients that an HBsAg level of <100IU/ml might predict lower risk of relapse after stopping NA treatment. In clinical practice, serum HBsAg level should be used together with, but not as a substitute for, HBV DNA., (Copyright © 2011 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published
2011
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12. HBsAg level at time of liver transplantation determines HBsAg decrease and anti-HBs increase and affects HBV DNA decrease during early immunoglobulin administration.

Author

Rosenau J, Kreutz T, Kujawa M, Bahr MJ, Rifai K, Hooman N, Finger A, Michel G, Nashan B, Kuse ER, Klempnauer J, Tillmann HL, and Manns MP

Subjects
Adult, Dose-Response Relationship, Drug, Drug Administration Schedule, Female, Follow-Up Studies, Hepatitis B prevention & control, Humans, Immunization, Passive, Immunoglobulins therapeutic use, Kinetics, Male, Middle Aged, Secondary Prevention, DNA, Viral blood, Hepatitis B Antibodies blood, Hepatitis B Surface Antigens blood, Hepatitis B virus genetics, Immunoglobulins administration & dosage, Liver Transplantation immunology, Postoperative Care
Abstract

Background/aims: Administration of hepatitis B immunoglobulin (HBIG) initially after liver transplantation of hepatitis B patients is considered important to prevent reinfection reliably. However, dosing schedules differ considerably between centers. We measured HBsAg, anti-HBs and HBV DNA kinetics to create a rational basis for dosing schemes., Methods: Thirteen patients (group A) received 10,000 IU HBIG in the anhepatic phase followed by 10,000 IU daily until HBsAg became negative, whereas five patients (group B) received 20,000 IU followed by 5000 IU every 30 min., Results: HBsAg levels at time of transplantation ranged from 0.12 to 12,990 IU/ml. Correlations between initial HBsAg and HBIG required to decrease HBsAg below 1 IU/ml were high in groups A and B (r=0.97, p<0.001; r=1.00, p<0.001), as were correlations between initial HBsAg and HBIG required to raise anti-HBs above 1000 IU/l (r=0.94, p<0.001; r=1.00, p<0.001). In 11 HBV DNA-positive patients, DNA levels became negative in seven, and dropped by 2.5 log10 (mean) in the other four patients during immunoglobulin administration., Conclusions: In conclusion, required HBIG doses to decrease HBsAg and raise anti-HBs are determined by HBsAg levels at time of transplantation, not by HBV DNA levels. Shortened HBIG dosing intervals accelerate HBsAg decrease and anti-HBs increase. HBV DNA decreases rapidly during HBIG administration in most patients.

Published
2007
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13. Hepatitis A virus infection suppresses hepatitis C virus replication and may lead to clearance of HCV.

Author

Deterding K, Tegtmeyer B, Cornberg M, Hadem J, Potthoff A, Böker KH, Tillmann HL, Manns MP, and Wedemeyer H

Subjects
Acute Disease, Adult, Aged, Disease Progression, Female, Follow-Up Studies, Hepatitis A complications, Hepatitis A Antibodies immunology, Hepatitis A virus genetics, Hepatitis A virus immunology, Hepatitis C complications, Hepatitis C Antibodies immunology, Humans, Male, Middle Aged, Polymerase Chain Reaction, RNA, Viral genetics, Retrospective Studies, Time Factors, Hepacivirus physiology, Hepatitis A virology, Hepatitis C virology, Superinfection virology, Viral Interference, Virus Replication physiology
Abstract

Background/aims: The significance of hepatitis A virus (HAV) super-infection in patients with chronic hepatitis C had been a matter of debate. While some studies suggested an incidence of fulminant hepatitis A of up to 35%, this could not be confirmed by others., Methods: We identified 17 anti-HCV-positive patients with acute hepatitis A from a cohort of 3170 anti-HCV-positive patients recruited at a single center over a period of 12 years., Results: Importantly, none of the anti-HCV-positive patients had a fulminant course of hepatitis A. HCV-RNA was detected by PCR in 84% of the anti-HCV-positive/anti-HAV-IgM-negative patients but only in 65% of anti-HCV-positive patients with acute hepatitis A (p=0.03), indicating suppression of HCV replication during hepatitis A. Previous HAV infection had no effect on HCV replication. After recovery from hepatitis A, an increased HCV replication could be demonstrated for 6 out of 9 patients with serial quantitative HCV-RNA values available while 2 patients remained HCV-RNA negative after clearance of HAV throughout follow-up of at least 2 years., Conclusions: HAV super-infection is associated with decreased HCV-RNA replication which may lead to recovery from HCV in some individuals. Fulminant hepatitis A is not frequent in patients with chronic hepatitis C recruited at a tertiary referral center.

Published
2006
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14. Famciclovir treatment of chronic delta hepatitis.

Author

Yurdaydin C, Bozkaya H, Gürel S, Tillmann HL, Aslan N, Okçu-Heper A, Erden E, Yalçin K, Iliman N, Uzunalimoglu O, Manns MP, and Bozdayi AM

Subjects
Adult, Biopsy, Famciclovir, Female, Hepatitis D, Chronic pathology, Hepatitis Delta Virus genetics, Humans, Liver pathology, Liver virology, Male, Middle Aged, Pilot Projects, RNA, Viral analysis, 2-Aminopurine administration & dosage, 2-Aminopurine analogs & derivatives, Antiviral Agents administration & dosage, Hepatitis D, Chronic drug therapy, Hepatitis Delta Virus isolation & purification
Abstract

Background/aims: Interferon is the only established therapy for chronic delta hepatitis and alternative treatment options are an urgent need. Since successful treatment of a case of post-transplant delta hepatitis with the nucleoside analogue famciclovir had been reported, a pilot study was undertaken to evaluate the use of famciclovir in the treatment of chronic delta hepatitis., Methods: A total of 15 adult patients, 13 men, two women, ages 20-52 years, with chronic delta hepatitis were treated with famciclovir, 500 mg, three times a day for 6 months and were then followed-up for 6 months posttreatment. All patients had compensated chronic liver disease, elevated liver enzymes and were hepatitis delta virus (HDV) RNA positive by polymerase chain reaction at baseline. Patients were monitored and tested for HBsAg, hepatitis B virus (HBV) DNA and HDV RNA levels. Liver biopsies were obtained before starting famciclovir and within 1 month of completion of treatment., Results: HBV DNA levels decreased in nine of the 15 patients and levels rose again after treatment (P<0.05). Famciclovir had no effect on alanine aminotransferase (ALT) and HBsAg levels or on serum HDV RNA and overall, there was no improvement in liver histology., Conclusions: Treatment of chronic delta hepatitis with famciclovir has no effect on disease activity and HDV RNA levels.

Published
2002
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